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www.doh.dc.govwww.doh.dc.gov
Medical Cannabis and Pain
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Collaborators
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More resources available at theDC Center for Rational Prescribing
doh.dc.gov/dcrx
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• Donald I. Abrams, MD
• Adriane Fugh-Berman, MD
• Mikhail Kogan, MD
• Susan Wood, PhD
Course Faculty
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Important Information
The video will progress at its own pace.
Do not attempt to speed up the video.
The post-test will only unlock after viewing the entire video.
The video can be paused and resumed later.
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Course Objectives
After completing this module, participants should be able to…
Differentiate characteristics of cannabinoid receptors.
List three appropriate uses for medical cannabis.
Compare advantages and disadvantages of different routes of cannabis administration.
Describe the relationship between opioids and cannabinoids.
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Cannabis and Pain
Donald I. Abrams, MDChief, Hematology-OncologyZuckerberg Francisco General HospitalProfessor of Clinical Medicine, UCSF
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Conflicts of Interest
Dr. Donald Abrams discloses that he has financial relationships with the following companies.
• ABcann• AXIM Biotechnologies, Inc• Maui Wellness Group• Scriptyx• Tikun Olam
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Cannabis as Medicine
• Marijuana (cannabis, hemp) is one of the oldest known psychoactive plants
• First reported use as medicine ~3,000 years ago
• Introduced into Western medicine in 1840s by Dr. W.B. O’Shaughnessy
• Promoted for putative analgesic, sedative, anti-inflammatory, antispasmodic and anticonvulsant properties
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Additional products available in 1906manufactured by Eli Lilly, Wyeth, Sharp & Dohme
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Cannabis as Medicine
• Interest waned in early 1900s with advent of opiates, barbiturates, chloral hydrate, aspirin and syringes
• First federal restrictions in 1937 with Marihuana Tax Act ($1/oz for medical use, $100/oz for recreational users)
• AMA was virtually alone in opposing act.
• Believed objective data re: harmful effects were lacking
• Act would impede future clinical investigations
• Removed from US Pharmacopoeia in 1942
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Stakeholder Meeting for the National Academies’ Report:
The Health Effects of Cannabis and Cannabinoids:
The Current State of Evidence and Recommendations for Research
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Cannabinoid Receptors
• CB1 and CB2 receptors identified
• Receptors encoded by separate genes on separate chromosomes; share 48% amino acid identity
• G-protein coupled receptors that inhibit adenylyl cyclase on activation
• Decreases cyclic AMP and protein kinase A activity
• Inhibition of Ca++ influx through various Ca++ channels
• Stimulation of inwardly rectifying K+ channels and mitogen-activated protein kinase cascades
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Cannabinoid1 Receptor
• CB1 receptors identified throughout central and peripheral nervous system• Density highest in cingulate gyrus, frontal cortex, hippocampus, cerebellum and
basal ganglia
• CB1 receptors present in virtually all organs and tissues of the body
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Cannabinoid2 Receptor
• CB2 receptor originally detected in macrophages and marginal zone of the spleen
• Largest concentration in peripheral blood present in B-cells and NK cells
• Also found in bone and to a lesser degree in liver and nerve cells
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Endocannabinoids
Anandamide
NH
O
OH
Docosatetraenoylethanolamide
O
NH
OH
NH
O
OH
Di-homo--linolenoylethanolamide
O
OOH
OH
2-Arachidonyl-Glycerol
CB1
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CB1 receptor
Pre-synaptic terminal
Post-synaptic terminal
Neurotransmitter vesicles
AA
ETA
AEA
MA
GL
AA
Glycerol
Neurotransmitter receptor
STOPSTOP
Neurotransmitterreceptor
DAGL NAPE
DAG
THCDronabinolNabilone
THCDronabinolNabilone
Ca2+
-K+
Ca2+
K+
+CB1 receptor
2-AG
2-AG2-AG
AEA
1
1
22
33
44
55
6
6
Health Canada 2016
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CB1 receptor
Pre-synaptic terminal
Post-synaptic terminal
Neurotransmitter vesicles
AA
ETA
AEA
MA
GL
AA
Glycerol
Neurotransmitter receptor
STOPSTOP
Neurotransmitterreceptor
DAGL NAPE
DAG
THCDronabinolNabilone
THCDronabinolNabilone
Ca2+
-K+
Ca2+
K+
+CB1 receptor
2-AG
2-AG2-AG
AEA
1
1
22
33
44
55
6
6
Serotonin (5-HT) Glutamate Acetylcholine
GABA Noradrenaline Dopamine
D-aspartate Cholecystokinin
Health Canada 2016
Suppression of Neurotransmitter Release
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Endogenous Cannabinoid System
CB1 Receptor
R
O
Endocannabinoids
Signal Transduction
Appetite Cognition Immune function EmesisMuscle control NeuroexcitabilityPain RewardIOP Thermoregulation
SynthesisMetabolism
Cellular uptake
CB2 Receptor CBx Receptor VR1 Receptor
Immune functionCell proliferationInflammationPain
PainVaso-dilation
PainInflammation
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Cannabinoids and Pain
• Elevated levels of the CB1 receptor – like the opioid receptor – are found in areas of the brain that modulate nocioceptive processing
• CB1 and CB2 agonists have peripheral analgesic actions.
• CBs may also exert anti-inflammatory effects
• Analgesic effects not blocked by opioid antagonists
• Effective in rodent model of neuropathic pain
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Experimental Pain Model
Pain model timeline: Days 1 and 5
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Results: Neurology RCT
Abrams 2007
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Results: Neurology RCT
Abrams 2007
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Results: Neurology RCT
Abrams 2007
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Results: Neurology RCT
Abrams 2007
Cannabis
Placebo
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Results: Neurology RCT
Abrams 2007
Cannabis
Placebo
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Results: Neurology RCT
Abrams 2007
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Cannabinoid: Opioid Interactions
Effects of cannabinoids in mice and rats
• THC enhances analgesic effect of morphine in a synergistic fashion
• Oral-Δ-9-THC increases potency of other mu opioids (hydromorphone and oxymorphone)
• Cannabinoids may enhance of analgesic effect of opioids
• The same analgesic effect may be achieved at lower opioid doses.
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• Funded by the National Institute on Drug Abuse (NIDA)
• Published 2 November 2011 in Clinical Pharmacology & Therapeutics
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Cannabinoid-Opioid Interaction TrialObjectives
• Evaluate effects of vaporized cannabis on blood levels of prescribed opioids
• Sustained-release morphine
• Sustained-release oxycodone
• Determine the short-term side effects of co-administration of cannabis and opioids
• Assess effect of vaporized cannabis on level of chronic pain
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Participant Characteristics
Morphine Oxycodone
10 Number Enrolled 11
4 Women 6
8 Caucasian 9
42.9 (33-55) Age 47.1 (28-61)
62 mg bid
(10-200)
Opioid Dose 53 mg bid
(10-120)
34.8
(29.4, 40.1)
Pain Score day 1 43.8
(38.6, 49.1)
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0
20
40
60
80
100
0 1 2 4 6 8 10 12
Hour
Ox
yc
od
on
e p
las
ma
le
ve
l
(mg
/ml)
Day 1 Day 5
b. Oxycodone
Plasma Opiate Levels by Study Day
0
20
40
60
80
100
0 1 2 4 6 8 10 12
Hour
Mo
rph
ine
pla
sm
a l
ev
el
(mg
/ml)
Day 1 Day 5
a. Morphine
Abrams 2011
Morphine Group Oxycodone Group
Cannabinoids did not significantly change the plasma level of opioids
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Pain by Study Day
n
Day 1
Mean
(95% CI)
Day 5
Mean
(95% CI)
Difference
Mean
(95% CI)*
Overall 21 39.6
(35.8, 43.3)
29.1
(25.4, 32.8)
-10.7
(-14.4, -7.3)
Morphine 10 34.8
(29.4, 40.1)
24.1
(18.8, 29.4)
-11.2
(-16.5, -6.0)
Oxycodone 11 43.8
(38.6, 49.1)
33.6
(28.5, 38.6)
-10.3
(-14.8, -5.8)
*p<0.001
Abrams 2011
www.doh.dc.gov
Pain by Study Day
n
Day 1
Mean
(95% CI)
Day 5
Mean
(95% CI)
Difference
Mean
(95% CI)*
Overall 21 39.6
(35.8, 43.3)
29.1
(25.4, 32.8)
-10.7
(-14.4, -7.3)
Morphine 10 34.8
(29.4, 40.1)
24.1
(18.8, 29.4)
-11.2
(-16.5, -6.0)
Oxycodone 11 43.8
(38.6, 49.1)
33.6
(28.5, 38.6)
-10.3
(-14.8, -5.8)
*p<0.001
Abrams 2011
www.doh.dc.gov
Pain by Study Day
n
Day 1
Mean
(95% CI)
Day 5
Mean
(95% CI)
Difference
Mean
(95% CI)*
Overall 21 39.6
(35.8, 43.3)
29.1
(25.4, 32.8)
-10.7
(-14.4, -7.3)
Morphine 10 34.8
(29.4, 40.1)
24.1
(18.8, 29.4)
-11.2
(-16.5, -6.0)
Oxycodone 11 43.8
(38.6, 49.1)
33.6
(28.5, 38.6)
-10.3
(-14.8, -5.8)
*p<0.001
Abrams 2011
32.1% reduction
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Pain by Study Day
n
Day 1
Mean
(95% CI)
Day 5
Mean
(95% CI)
Difference
Mean
(95% CI)*
Overall 21 39.6
(35.8, 43.3)
29.1
(25.4, 32.8)
-10.7
(-14.4, -7.3)
Morphine 10 34.8
(29.4, 40.1)
24.1
(18.8, 29.4)
-11.2
(-16.5, -6.0)
Oxycodone 11 43.8
(38.6, 49.1)
33.6
(28.5, 38.6)
-10.3
(-14.8, -5.8)
*p<0.001
Abrams 2011
32.1% reduction
23.5% reduction
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Conclusions
Co-administration of vaporized cannabis with oral sustained-release opioids is safe
Co-administration of vaporized cannabis trends towards lowering concentration of the opioids
• The PK effects would be expected to reduce the analgesic effects of the opioids
• The effect of vaporized cannabis to enhance opioid analgesia occurs by a pharmacodynamic, not a pharmacokinetic mechanism
Co-administration of vaporized cannabis in subjects on stable dose of morphine or oxycodone appears to enhance analgesia
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Therapeutics
• In adults with chemotherapy-induced nausea and vomiting, oral cannabinoids are effective antiemetics.
• In adults with chronic pain, patients who were treated with cannabis or cannabinoids were more likely to experience a clinically significant reduction in pain symptoms.
• In adults with multiple sclerosis-related spasticity, short-term use of oral cannabinoids improves patient-reported spasticity symptoms.
• For these conditions, the effects of cannabinoids are modest; for all other conditions evaluated there is inadequate information to assess benefits.
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The Safety of Cannabis
• No overdose deaths have been reported.
• An estimated 800 cigarettes would be required to kill
• Death would be from CO poisoning
• Unlike opioid receptors, dearth of brainstem cannabinoid receptors
• Addictive potential and minor withdrawal syndrome less than or equal to caffeine
Grothenherman 2002
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Cannabis and Pain:DC Experience
Mikhail Kogan, MDMedical DirectorGW Center for Integrative MedicineAssistant Professor of MedicineAssociate Director of Geriatric and Integrative Medicine FellowshipsGeorge Washington University
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Conflicts of Interest
• Dr. Mikhail Kogan did not disclose any financial conflicts of interest.
• Dr. Kogan does recommend Medical Cannabis to patients in DC.
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Case: Middle aged man withchemotherapy induced neuropathyPatient
• 59 year old man survival of colon cancer treated with surgery and chemo.
• Severe Chemotherapy induced neuropathy for months. Tried number of medications with partial response and number of side effects.
• Primary care doctor and oncologist refused to recommend cannabis citing lack of evidence and not participating in DC Medical Cannabis program.
• Other symptoms: Weight loss, Poor appetite “food does not taste good”
• BMI on 1st visit 18.5
Goals
Control pain and gain some weight
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Case: Middle aged man withchemotherapy induced neuropathyPatient
• 59 year old man survival of colon cancer treated with surgery and chemo.
• Severe Chemotherapy induced neuropathy for months. Tried number of medications with partial response and number of side effects.
• Primary care doctor and oncologist refused to recommend cannabis citing lack of evidence and not participating in DC Medical Cannabis program.
• Other symptoms: Weight loss, Poor appetite “food does not taste good”
• BMI on 1st visit 18.5
Goals
Control pain and gain some weight
8 weeks after recommendation
• Gained 5 lbs, no side effects, reports use twice daily with vaporizer, pain is mostly controlled, occasionally needs to use extra few doses/day.
• Tolerating euphoria well and the only problem – COST but “it is worth it”
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Clinical Side of Recommending Cannabis:Philosophy and Logistics
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THC: TetrahydrocannabinolBeyond Psychoactive Effects
Anti-inflammatory
Anti-emeticAnalgesic
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CBD: CannabidiolNon Psychoactive cannabinoid
Non psychoactive, discovered in 1963
Modulates THC effects, low affinity to CB1 and CB2 receptors
Potent P450 3A11 inhibitor – blocking formation of most psychoativemetabolite of THC – 11-OH
Sedative properties – reduces anxiety and other negative THC side effect
Mild analgesic effects
Anti-inflammatory
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Non Psychotropic Cannabinoids
Izzo 2009
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Chronic Pain
A systematic review of 18 randomized controlled trials (RCTs) with a total of 766 participants with chronic non-cancer pain found that 15/18 trials showed a significant analgesic effect of cannabinoids, compared to placebo.
• Conditions studied included neuropathic pain, “chronic pain,” rheumatoid arthritis, fibromyalgia, and central pain in multiple sclerosis.
• No serious adverse events were reported.
Lynch and Campbell 2011
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Chronic Pain
A systematic review identified 28 studies (27 placebo-controlled, 1 treatment-controlled) of cannabis in a total of 2,454 participants with chronic pain.
Whiting 2015
• 12 studies of neuropathic pain
• 6 trials of other types of pain
• 3 for cancer pain
• 3 for diabetic neuropathy
• 2 for fibromyalgia
• 2 for HIV-associated sensory neuropathy
Preparations tested included nabiximols, nabilone, inhaled cannabis, THC (oral or oralmucosal), and dronabinol.
Studies generally showed improvements in pain measures with cannabis and cannabinoids.
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Chronic Pain Neuropathic Pain
STUDY POPULATION TREATMENT OUTCOME
Abrams (2007)
RCT (parallel group) in 55 patients with HIV-associated neuropathy.
Smoked cannabis (3.56% THC) or placebo cigarettes without cannabinoids 3 times/day for 5 days.
Smoked cannabis reduced daily pain by 34% vs. 17% in placebo group (p=0.03); greater than 30% reduction in pain was reported by 52% in cannabis group vs. 24% in control (p=0.04). The first cigarette reduced chronic pain by 72% in cannabis group vs. 15% in control (p<.001).
Ellis (2009)RCT (crossover) in 34 patients with HIV-associated neuropathy.
Cannabis (1-8% THC) or placebo 4 times/dayfor 5 consecutive days/week for two weeks.
The proportion with pain reduction greater than 30% was 0.46 with cannabis vs. 0.18 with placebo; pain reduction was greater with cannabis than placebo (p=.016).
GW Pharma Ltd (2005)
RCT (parallel group) in 297 patients with diabetic peripheral neuropathy.
Nabiximols (Sativex) or placebo up to 24 sprays/day over 14 weeks.
There was no benefit of nabiximols over placebo in proportion of patients with pain reduction greater than 30%.
Selvarajah(2010)
RCT (parallel group) in 30 patients with diabetic peripheral neuropathy.
Nabiximols (Sativex) or placebo up to 4 sprays/day over 2 weeks.
There was no benefit of nabiximols over placebo on mean daily pain scores.
Wallace (2013)
RCT (crossover) in 16 patients with diabetic peripheral neuropathy.
Oromucosal spray (1%, 4%, and 7% THC) or placebo in single doses
There was a significant difference between placebo and all doses (p<.05) for spontaneous pain. High doses were significantly better than low/medium doses (p=.001). Only high doses were effective for evoked pain (p<.001).
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Chronic Pain Neuropathic Pain
STUDY POPULATION TREATMENT OUTCOME
Berman (2007)
RCT (crossover) in 117 patients with central neuropathic pain (non-acute spinal cord injury). (unpublished abstract of conference presentation)
Nabiximols (Sativex) (2.7 mg THC and 2.5 mg CBD); THC spray, or placebo up to 48 sprays/24 h for 2 weeks each.
There was no difference between nabiximols (Sativex) and placebo for NRS pain scores.
Berman (2004)
RCT (crossover) in 48 patients with central neuropathic pain (brachial plexus avulsion)
Nabiximols (Sativex) (2.7 mg THC and 2.5 mg CBD); THC spray, or placebo up to 48 sprays/24 h for 2 weeks each.
Nabiximols (Sativex) was superior to placebo in reduction in pain score (by diary entry (p<.005).
Frank (2008)RCT (crossover) in 96 patients with mixed neuropathic pain
Dihydrocodeine (30mg-240mg) or nabilone (250 mcg-2mg) for 7 weeks each.
Dihydrocodeine was significantly better than nabilone as measured by the visual analogue score (VAS) (p=.01).
Karst (2003)RCT (crossover) in 21 patients with chronic neuropathic pain
CT-3 (a synthetic cannabinoid) 20 mg orally or placebo 2x/day for 4 days, then 40 mg 2x/day for 3 days.
Treatment and placebo in pain measured by visual analog scale 3hours after intake, but differences were less pronounced after 8 hours (p=.02).
Langford (2013)
RCT (parallel group) in 339 patients with central neuropathic pain due to MS
THC/CBD spray (2.7 mg THC and 2.5 mg CBD) or placebo, self-titrated for 14 weeks.
THC/CBD spray was not superior to placebo in mean NRS pain score.
Nurmikko(2007)
RCT (parallel) in 125 patients with neuropathic pain characterized by allodynia
Nabiximols spray (2.7 mg THC and 2.5 mg CBD) up to 48 sprays/24 h for 7-10 days.
Nabiximols (Sativex) was superior to placebo in mean reduction in pain intensity scores by VAS (p=.004)
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Chronic Pain Neuropathic Pain
Cannabinoids are effective for the treatment of pain, especially neuropathic pain.
Another systematic review and meta-analysis of 18 double blind randomized placebo-controlled trials of cannabis and cannabinoid treatments for chronic pain also showed that cannabis and cannabinoids appear to reduce pain intensity. Martin-Sanchez 2009
6 double-blind randomized controlled trials (n=226) studied the use of medical cannabis in neuropathic pain. All studies showed a statistically significant benefit in terms of pain relief. Deshpande 2015
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Case: Peripheral Neuropathy in Elderly Woman
Patient
• 76 year old frail woman with diabetes-related peripheral neuropathy and chronic kidney disease admitted to the hospital ICU with severe delirium.
• 7 days before admission, gabapentin dose was increased to 300mg every 8 hours.
• Geriatrics consult was called. Gabapentin was rapidly tapered down and delirium slowly resolved.
Outpatient treatment
• Weekly acupuncture
• Finished gabapentin taper
• Combination of alpha-lipoicacid, benfotiamine, and GLA (evening primrose oil)
• Medical cannabis recommendation – sublingual tincture as needed
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Case – 12 weeks follow up
• “Well I did get very a high few times, reminded me of my hippie years. After few weeks I figured out how to dose it just right.”
• “I have no idea if supplements are doing anything but acupuncture has been somewhat helpful.”
• “I have to choose pot over acupuncture, all these costs add up.”
• “Can’t you write me some letter for Medicare? I mean why all your effective treatments are not covered, while the medication that almost killed me is?”
• “Oh, and my primary care doctor wants you to call him. He thinks I should not use pot as it is very dangerous at my age and he wants to put me on another medication instead, but I don’t think so.”
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Cannabis Toxicity/Addiction
Gable 2006
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Cannabis Toxicity/Addiction
Gable 2006
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Acute Pain
RCTs have shown:
Cannabis and cannabinoids are not recommended for acute pain.
• No effect of intravenous THC on dental extraction pain. Raft 1977
• No effect of THC capsules or sublingual spray on post-operative pain after abdominal hysterectomy. Buggy 2003
• Levonantradol* was shown to be no more effective than codeine for acute post-operative pain. Campbell 2001
*Levonantradol is a synthetic, potent analog of THC, usually given intramuscularly. Levonantradol is no longer used clinically.
www.doh.dc.gov64
Administration and Formulations
(herbal cannabis, resin, concentrates)
Inhalation by smoking or
vaporization
(prescription cannabinoids,
edibles, tinctures)
Oral
(lollipops, lozenges,
nabiximols)
Oro-mucosal or sublingual
(herbal cannabis, resin, concentrates)
Topical or Rectal
www.doh.dc.gov
Cannabis vs. Cannabinoids
Advantages of cannabinoids
• High quality control
• No variability between batches
• Possibly insurance coverage
For both cannabis and cannabinoids, “Start low and go slow.”
Advantages of cannabis
• Many clinicians believe cannabis has a different effect than synthesized cannabinoids.
• Cannabis has many different cannabinoid and non-cannabinoid constituents that may work synergistically (the so-called “entourage effect”).
• Cannabis is less expensive than prescription forms.
• It is much easier to slowly and precisely titrate the dose.
• Typically there are fewer side effects, mostly due to the of presence of CBD and avoiding oral administration.
www.doh.dc.gov
Smoking
• A “joint” contains 0.5 - 0.8 g of cannabis with about 4 - 8% THC, but many strains now are much stronger.
• About 20 - 70% of that ~ 5 mg of THC reaches the lungs
• About 30% of THC and CBD is bioavailable
• Plasma peaks of THC occur in 3 to 10 minutes.
• Plasma clears in about 3 hours, the high usually lasts about 1 to 2 hours, sometimes up to 4 hours.
The Pot Book 2010
www.doh.dc.gov
Vaporizing
Pros• Much lower temperature
• Minimal particulate matter
• Less carbon monoxide
• Better THC delivery compared to smoking due to loss of THC at high temperature
• Lower risk of accidental burn injuries or fires
• Some are easy to use (pen oil vaporizers)
Cons• Need special equipment
• Higher cost (ranges from $50 - 500)
• Some more difficult to use
• Long term risks of inhaling vaporized oils are unknown
www.doh.dc.gov
Oral and Sublingual Use of Whole Plant Extracts
• Oral administration
• Slow peak level and prolonged psychoactive effect
• No seizures or CNS suppression due to CBD counter effect at cannabinoid receptors, in contrast to pure THC products
• Oil and whole plant tinctures available for oral and sublingual use
• Some are very potent
• Per mg cost of active ingredients is often cheaper
• Often more stable
• Some commercial products have very high CBD:THC ratio and have minimal or no psychoactive effects
• In my experience, 8:1 CBD:THC ratio does not caused psychoactive side effects
www.doh.dc.gov
Patient
• 21 year old healthy college student on soccer scholarship
• Head trauma with loss of teeth and oral fractures during soccer
• Multiple oral and dental surgeries
• Referred by oral surgeon
On presentation to the clinic• Severe facial pain mostly in lower jaw, upper neck, and
headaches
• Frequent and severe flares, responding best to intravenous ketamine infusion when admitted to the hospital. At times pain-free between flares.
• OxyContin and OxyIR with typical total oxycodone daily dose 120-150mg/day
• Sleep disrupted, anxiety, and depression with suicidal thoughts, weight gain of 30 lbs., craving sweets and alcohol
• Unable to exercise or play soccer, dropped out of college, moved back in with his parents
Case – Young patient with chronic facial pain
www.doh.dc.gov
Treatment plan
• Working with psychiatrist: antidepressant, mood stabilizer, weekly cognitive behavioral therapy (CBT), breathing and mindfulness practices
• Anti-inflammatory diet, fish oil, methylated B complex
• Acupuncture
• Gradual exercise and manual medicine with PT
• Twice a month low dose intravenous ketamine infusions
• Inhaled high-THC preparation as needed throughout the day and scheduled sublingual tincture of cannabis (1:1 THC:CBD ratio) whole plant extract at bedtime
Case – Young patient with chronic facial pain
www.doh.dc.gov
Case Progression
• Down to oxycodone 10 mg as needed, 30 tabs (used only during flares) lasted 2-3 months
• Decreased ketamine infusions frequently, stopped acupuncture
3 MO.
• Lost 30 lbs. of gained weight, slowly increased exercise (mostly walking and swimming)
• Depression lifted, started to taper off antidepressants
• Stopped all inhaled cannabis, occasionally uses sublingual tincture for sleep or for flares
6 MO.
www.doh.dc.gov
Qualifying Medical Conditions
In early years of law:
• DOs
• MDs
• NDs (recently added)
HIV-related cachexia, glaucoma, MS-relate spasticity, side effects from cancer treatments
Now:
Up to recommending physician to determine if patient has qualifying medical condition
Who can recommend?
www.doh.dc.gov
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What Recommenders Need to Know
• How to counsel patients about risks and benefits
• How to pick the right strain
• Appropriate ratios of THC:CBD
• Effects of other cannabinoids
• What are the routes of administration I should suggest?
• How much can I rely on a medical cannabis dispensary to educate my patients?
www.doh.dc.gov
Resources
For more information on prescribing in the District and to become a recommending physician visit:
Please visit DCRx for a full list of references and more information on these and other treatment-related subjects.
Questions can be sent by email to [email protected] or by regular mail to:
Medical Marijuana ProgramHealth Regulation and Licensing Administration899 N. Capitol Street, NE2nd FloorWashington, DC 20002
doh.dc.gov/mmp doh.dc.gov/dcrx
www.doh.dc.gov
Audience Questions
www.doh.dc.gov
Do you have any experience recommending cannabis for
patients who are weaning off of opioids?
www.doh.dc.gov
Does cannabis work for all types of chronic pain, i.e. back pain,
fibromyalgia, arthritis?
www.doh.dc.gov
Is there any difference in reimbursement between
California and DC?
www.doh.dc.gov
How do you treat chronic pain patients who are also being treated
with antipsychotics, antidepressants, or mood
stabilizers?
www.doh.dc.gov
Would you recommend cannabis for pregnant patients dealing with
chronic pain?
www.doh.dc.gov
Do you recommend cannabis to patients who have a history of
addiction or substance use disorder?
www.doh.dc.gov
More resources available at the
DC Center for Rational Prescribing
doh.dc.gov/dcrx
www.doh.dc.gov
Medical Cannabis: An Introduction to the Biochemistry & Pharmacology
Medical Cannabis: Evidence on Efficacy
Medical Cannabis: Adverse Effects and Drug Interactions
Rational Prescribing in Older Adults
Drug Approval and Promotion in the United States
Generic Drugs: Myths and Facts
DCRx Modules
Getting Patients Off of OpioidsMyths and Facts about Opioids
Taking a Sexual History to Reduce HIV RiskWhat You Need to Know about PrEP
Industry Influence on the Practice of Medicine
Tight Control in Type 2 Diabetes: More Harm Than Good?